EP2411006B1 - Zusammensetzungen und verfahren zur behandlung von nierenkrankheit - Google Patents
Zusammensetzungen und verfahren zur behandlung von nierenkrankheit Download PDFInfo
- Publication number
- EP2411006B1 EP2411006B1 EP10756917.0A EP10756917A EP2411006B1 EP 2411006 B1 EP2411006 B1 EP 2411006B1 EP 10756917 A EP10756917 A EP 10756917A EP 2411006 B1 EP2411006 B1 EP 2411006B1
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- EP
- European Patent Office
- Prior art keywords
- agent
- aldosterone
- diabetes
- indapamide
- proteinuria
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Definitions
- the invention relates to methods and compositions related to the treatment of subjects with proteinuria and/or hypertension (e.g., proteinuria and/or hypertension arising from primary renal disease or secondary to other conditions (e.g., diabetes, diabetic nephropathy, liver disease).
- proteinuria and/or hypertension e.g., proteinuria and/or hypertension arising from primary renal disease or secondary to other conditions (e.g., diabetes, diabetic nephropathy, liver disease).
- an indoline i.e., indapamide
- an anti-aldosterone agent e.g., spironolactone and/or eplerenone
- Diabetes mellitus is one of the leading causes of morbidity and mortality in the United States because of its role in the development of ophthalamic, renal, neuropathic, and cardiovascular disease. These complications, particularly cardiovascular disease ( ⁇ 50-75% of medical expenditures), are the major sources of expense and suffering for patients with diabetes mellitus. Approximately two thirds of people with diabetes die from heart disease or stroke. Men with diabetes face a 2-fold increased risk for coronary heart disease, and women have a 3-to 4-fold increased risk. In 1994, 1 of every 7 health care dollars in the United States was spent on patients with diabetes mellitus. The 2002 estimate for direct medical costs due to diabetes in the United States was $92 billion, with another $40 billion in indirect costs. Approximately 20% of Medicare funds are spent on patients with diabetes.
- Diabetic nephropathy affects approximately 20-40% of all individuals with diabetes ( American Diabetes Association (2009) Diabetes Care 32:S13-S61 ) and is the single most common cause of end-stage renal disease (ESRD) in the United States, leading to the need for dialysis.
- ESRD end-stage renal disease
- Risk for the development of diabetic nephropathy is directly related to the cumulative duration and severity of hyperglycemia ( Wingard et al. (1993) Diabetes Care 16:1022-1025 ; herein incorporated by reference in its entirety), as well as the cumulative duration and severity of hypertension that commonly accompanies diabetes mellitus ( Raile et al. (2007) Diabetes Care 30:2523-2528 ;) although other non-modifiable risk factors such as age and genetic background also influence that risk.
- Renal damage in diabetes involves proteinuria of glomerular origin. Renal tubules of the kidneys retain plasma proteins by reabsorption of such proteins as they pass through the glomerular filtration barrier. Normal urine protein excretion is up to 150 mg/d. Therefore, the detection of abnormal quantities or types of protein in the urine is considered an early sign of significant renal or systemic disease. When proteinuria occurs, it can cause further renal damage through release of cytokines, inflammation of the renal tubulointerstitium, and progressive fibrosis.
- proliferative glomerulonephritis e.g., immunoglobulin A nephropathy, membranoproliferative glomerulonephritis, mesangial proliferative glomerulonephritis, anti-GBM disease, renal vasculitis, lupus nephritis, cryoglobulinemia-associated glomerulonephritis, bacterial endocarditis, Henoch-Schönlein purpura, postinfectious glomerulonephritis, hepatitis C), and nonproliferative glomerulonephritis (e.g., membranous glomerulonephritis, minimal-change disease, primary focal segmental glomerulosclerosis (FSGS), fibrillary glomerulone
- FGS focal segmental glomerulosclerosis
- BEAUFILS ET AL "Nephroangiosclerose” EMC - NEPHROLOGIE ELSEVIER, vol. 2, no. 3,1 August 2005, pages 103-124, XP027827841, ISSN: 1638-6248 ; BIANCHI S ET AL: "Long-term effects if spironolactone on proteinuria and kidney function in patients with chronic kidney disease" KIDNEY INTERNATIONAL, vol. 70, no.
- compositions comprising anti-aldosterone agents such as spironolactone.
- WO 00/27380 A2 (G.D. SEARLE &CO. ET AL.) 18 May 2000 and WO 96/24373 A2 (G:D: SEARLE & CO. ET AL.) 15. August 1996 disclose compositions comprising spironolactone and an ACE inhibitor.
- PUIG ET AL "Efficacy of indapamide SR Compared With Enalapril in Elderly Hypertensive Patients With Type 2 Diabetes", AMERICAN JOURNAL OF HYPERTENSION, NATURE PUBLISHING GROUP, UNITED STATES, vol. 20, no.
- the present invention relates to the use of compositions and to compositions related to the treatment of subject with proteinuria, albuminuria or hyperuricemia.
- the invention relates to the use of an indoline (i.e., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone or eplerenone).
- an indoline i.e., indapamide
- an anti-aldosterone agent e.g., spironolactone or eplerenone
- Renoprotection in patients suffering from or at risk for proteinuria is critical to prevent further kidney damage. Similarly, control of hypertension is also needed to prevent further proteinuria and the accompanying kidney damage.
- many of the currently available therapeutic agents for renoprotection and/or treatment of hypertension either provide limited renoprotection (especially over long periods of time, such as single ACE inhibitor or ARB agents that become ineffective due to "aldosterone escape"), or carry risk of other dangerous side effects such as electrolyte imbalance.
- renoprotective e.g., anti-proteinuria
- methods of the present description find use in the treatment of subjects with diabetes or a diabetes-related condition involving e.g., impaired glucose tolerance, impaired insulin sensitivity, impaired insulin production.
- diabetes-related condition involving e.g., impaired glucose tolerance, impaired insulin sensitivity, impaired insulin production.
- Such conditions and disease states include but are not limited to diabetes mellitus, type I diabetes, type II diabetes, gestational diabetes, metabolic syndrome, metabolic syndrome X, syndrome X, insulin resistance syndrome, Reaven's syndrome, CHAOS, and malnutrition-related diabetes mellitus.
- One of skill in the medical arts appreciates that such subjects are at increased risk of kidney disease and proteinuria, and that such subjects find benefit from renoprotective combination therapy, composition, method, and kits which are based on the present invention.
- methods of the present description find use in treatment of conditions or physiological states including but not limited to fluid retention, sodium retention, and hypertension (high blood pressure).
- combination therapies, compositions, methods, and kits of the present description find use in treating subjects with diseases or conditions causing or associated with proteinuria, including but not limited to diabetes and diabetes-related diseases (e.g., impaired insulin signaling, diabetes mellitus, type I diabetes, type II diabetes, gestational diabetes, metabolic syndrome, metabolic syndrome X, syndrome X, insulin resistance syndrome, Reaven's syndrome, CHAOS, and malnutrition-related diabetes mellitus), diabetic nephropathy, nephropathy, glomerular disease, liver disease, renal disease, membranous glomerulonephritis, severe cardiac failure, sleep apnea, nephrotic syndrome, drug-induced nephropathy, systemic lupus erythematosus, Goodpasture's syndrome, IgA nephropathy, Alport syndrome, acute post-streptococcal glomerulonephritis (PSGN), bacterial endocarditis, HIV-induced n
- diabetes-related diseases
- methods of the present description comprise testing a subject for proteinuria, followed by administering a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone).
- a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone).
- methods of the present invention comprise administering to a subject a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone), followed by testing the subject for proteinuria, followed by administering a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone), followed by a second round of testing for proteinuria.
- a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone)
- an anti-aldosterone agent e.g., spironolactone and/or eplerenone
- methods of the present invention comprise testing a subject for proteinuria, followed by administering a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone), followed by a second round of testing for proteinuria, and a second administration of a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone), with this second administration being modified in dose, duration, frequency, or administration route in a manner dependent upon the results of the prior testing.
- a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone)
- an anti-aldosterone agent
- the description comprises use of a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone) in the manufacture of a medicament for the treatment of a condition such as to diabetes and diabetes-related diseases (e.g., impaired insulin signaling, diabetes mellitus, type I diabetes, type II diabetes, gestational diabetes, metabolic syndrome, metabolic syndrome X, syndrome X, insulin resistance syndrome, Reaven's syndrome, CHAOS, and malnutrition-related diabetes mellitus), diabetic nephropathy, nephropathy, glomerular disease, liver disease, renal disease, membranous glomerulonephritis, severe cardiac failure, sleep apnea, nephrotic syndrome, drug-induced nephropathy, systemic lupus erythematosus, Goodpasture's syndrome, IgA n
- Methods of the present description are not limited by dosing, formulation, administration routes, or temporal administration regimens of the combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone).
- an indoline e.g., indapamide
- an anti-aldosterone agent e.g., spironolactone and/or eplerenone
- dosage of the indoline agent e.g., indapamide
- dosage of the indoline agent is in the range of about 0.25 mg up to about 2,000 mg per day, with variations necessarily occurring depending on the disease target, the patient, and the route of administration.
- dosages are administered orally in the range of about 0.05 mg/day to about 20 mg/day, more preferably in the range of about 0.05 mg/day to about 5 mg/day, most preferably in the range of about 0.05 mg/kg to about 0.2 mg per kg of body weight per day.
- dosage of the anti-aldosterone agent is in the range of about 2 mg up to about 2,000 mg per day, with variations necessarily occurring depending on the disease target, the patient, and the route of administration.
- dosages are administered orally in the range of about 0.05 mg/day to about 500 mg/day, more preferably in the range of about 0.05 mg/day to about 250 mg/day, most preferably in the range of about 0.05 mg/kg to about 0.2 mg per kg of body weight per day.
- Administration routes include but are not limited to oral, topical, and parenteral (e.g. intravenous, intramuscular, intraperitoneal, subcutaneous, intrathecal, intraarterial, nasal, or pulmonary administration). In preferred examples of the present disclosure, administration is oral.
- a combination therapy comprising an indoline (e.g., indapamide) administered in combination with an anti-aldosterone agent (e.g., spironolactone and/or eplerenone).
- an indoline e.g., indapamide
- an anti-aldosterone agent e.g., spironolactone and/or eplerenone
- the indoline agent e.g., indapamide
- anti-aldosterone agent e.g., spironolactone and/or eplerenone
- the combination therapy may be administered between 1 and 50 times per day, or less often (e.g., every other day, every three days, every 4 days, every 5 days, every 6 days, once a week, once a month, once every three months.)
- the combination therapy may be continued for 1 day, 1 week, 1 month, 1 year, 10 years, or more than 10 years.
- the agents are administered in combination using multiple delivery vehicles each of a single type (e.g., more than one type of delivery vehicle (e.g., pill, capsule, tablet) each with a single compound per delivery vehicle).
- the agents are administered in combination using a single delivery vehicle (e.g., pill, capsule, tablet) comprising more than one agent (e.g., an indoline agent (e.g., indapamide) and an anti-aldosterone agent in a single delivery vehicle (e.g., pill, capsule, tablet).
- a single delivery vehicle e.g., pill, capsule, tablet
- the agents are administered in combination in single delivery vehicle (e.g., pill, tablet, capsule) in further combination with other therapeutic agents (e.g., other active anti-hypertensive agents (e.g., one or more beta-blockers).
- combination therapies, compositions, methods, and kits of the present description find use in patients presenting with proteinuria and/or hypertension wherein proteinuria and/or hypertension remains uncontrolled despite prior or continued treatment with one or more other therapies (e.g., treatment with agents other than an indoline (e..g, indapamide) and an anti-aldosterone agent (e.g., spironolactone and/or eplerenone)).
- agents other than an indoline e..g, indapamide
- an anti-aldosterone agent e.g., spironolactone and/or eplerenone
- combination therapies, compositions, methods, and kits of the present invention find use in subpopulations of patients (e.g., ethnic minority and majority populations (e.g., African-American, Hispanic, Asian, Native American, multi-ethnic minority populations, populations distinguished by geographic ancestry, populations distinguished by culture, diet, climate, environmental exposures, etc)).
- subpopulations of patients for which combination therapies, compositions, methods, and kits of the present invention find use are identified on the basis of common biomarkers indicating shared geographical ancestry.
- the present disclosure provides a composition comprising an indoline, which is selected from indapamide and an anti-aldosterone agent, selected from spironolactone or eplerenone.
- an indoline which is selected from indapamide
- an anti-aldosterone agent selected from spironolactone or eplerenone.
- the indoline and the anti-aldosterone agent are formulated for simultaneous administration in a single delivery vehicle.
- the single delivery vehicle is formulated for oral administration.
- the present description provides a composition for use in a method for treating or preventing a condition such as proteinuria, albuminuria, hyperuricemia, in a subject comprising administering a combination therapy comprising an indoline and an anti-aldosterone agent.
- the indoline and the anti-aldosterone agent are administered as separate compositions.
- the indoline and the anti-aldosterone agent are administered as a single composition.
- the indoline is indapamide.
- the anti-aldosterone agent is an agent such as an aldosterone receptor blocker or an inhibitor of aldosterone synthesis.
- the aldosterone receptor blocker is an agent such as spironolactone or eplerenone.
- the indoline and the anti-aldosterone agent are formulated for simultaneous administration in a single delivery agent.
- the present description provides a method of treating a subject with a disease such as impaired insulin signaling, diabetes mellitus, type I diabetes, type II diabetes, gestational diabetes, metabolic syndrome, metabolic syndrome X, syndrome X, insulin resistance syndrome, Reaven's syndrome, CHAOS, malnutrition-related diabetes mellitus, diabetic nephropathy, nephropathy, glomerular disease, liver disease, renal disease, membranous glomerulonephritis, severe cardiac failure, nephrotic syndrome, systemic lupus erythematosus, Goodpasture's syndrome, IgA nephropathy, Alport syndrome, acute post-streptococcal glomerulonephritis (PSGN), bacterial endocarditis, HIV-induced nephropathy, glomerulosclerosis, focal segmental glomerulosclerosis (FSGS), membranous nephropathy (membranous glomerulopathy), obesity, minimal change disease (
- a disease such as
- the indoline is indapamide.
- the anti-aldosterone agent is an agent such as an aldosterone receptor blocker or an inhibitor of aldosterone synthesis.
- the aldosterone receptor blocker is an agent such as spironolactone or eplerenone.
- the indoline and the anti-aldosterone agent are formulated for simultaneous administration in a single delivery agent.
- the present description provides a method of promoting a state in a subject such as homeostasis of serum potassium level, homeostasis of serum uric acid level, normal cardiac ventricular rhythm, and/or normal QT interval comprising administering a composition comprising an indoline and an anti-aldosterone agent.
- the indoline is indapamide and the anti-aldosterone agent is an agent such as an aldosterone receptor blocker or an inhibitor of aldosterone synthesis.
- the method further comprises administration of an agent having a function such as preventing or reducing proteinuria, promoting natriuresis, and/or preventing or reducing hypertension.
- the agent is an agent such as an angiotensin converting enzyme inhibitor, an anti-renin agent, an endothelin antagonist, a calcium channel blocker, a beta blocker and/or an anti-inflammatory agent.
- the present description provides use of a combination therapy comprising an indoline and an anti-aldosterone agent for the treatment of a condition such as proteinuria, albuminuria, sodium retention, hypokalemia, hyperkalemia, hyperuricemia, dyslipidemia, or hyperglycemia in a subject.
- a condition such as proteinuria, albuminuria, sodium retention, hypokalemia, hyperkalemia, hyperuricemia, dyslipidemia, or hyperglycemia in a subject.
- the present description provides use of a combination therapy comprising an indoline and an anti-aldosterone agent for the treatment or prevention of a condition such as proteinuria, albuminuria, sodium retention, hypokalemia, hyperkalemia, hyperuricemia, dyslipidemia, or hyperglycemia in a subject comprising providing a subject suffering from or at risk for a condition such as proteinuria, albuminuria, sodium retention, hypokalemia, hyperkalemia, hyperuricemia, dyslipidemia, or hyperglycemia; providing the combination therapy comprising an indoline and an anti-aldosterone agent; and measuring a benefit related to a condition such as proteinuria, albuminuria, sodium retention, hypokalemia, hyperkalemia, hyperuricemia, dyslipidemia, or hyperglycemia.
- a condition such as proteinuria, albuminuria, sodium retention, hypokalemia, hyperkalemia, hyperuricemia, dyslipidemia, or hyperglycemia.
- the present description provides use of a combination therapy comprising an indoline and an anti-aldosterone agent for the treatment of a subject with a disease such as impaired insulin signaling, diabetes mellitus, type I diabetes, type II diabetes, gestational diabetes, metabolic syndrome, metabolic syndrome X, syndrome X, insulin resistance syndrome, Reaven's syndrome, CHAOS, malnutrition-related diabetes mellitus, diabetic nephropathy, nephropathy, glomerular disease, liver disease, renal disease, membranous glomerulonephritis, severe cardiac failure, nephrotic syndrome, systemic lupus erythematosus, Goodpasture's syndrome, IgA nephropathy, Alport syndrome, acute post-streptococcal glomerulonephritis (PSGN), bacterial endocarditis, HIV-induced nephropathy, glomerulosclerosis, focal segmental glomerulosclerosis (FSGS), membra disease such as impaired insulin signaling
- the present description provides use of a combination therapy comprising an indoline and an anti-aldosterone agent for the promotion of a state in a subject such as homeostasis of serum potassium level, homeostasis of serum uric acid level, normal cardiac ventricular rhythm, or normal QT interval comprising administering said composition comprising an indoline and an anti-aldosterone agent.
- the present description provides a composition comprising an indoline and an anti-aldosterone agent.
- Figure 1 shows a flowchart for methodology for a study comparing, e.g., a combination therapy of indapamide and spironolactone versus thiazide diuretic for additive control of albuminuria in diabetic nephropathy.
- the term “subject” refers to any animal (e.g., a mammal), including, but not limited to, humans, non-human primates, rodents, and the like, which is to be the recipient of a particular treatment.
- the terms “subject” and “patient” are used interchangeably herein in reference to a human subject.
- proteinuria refers to a condition in which excess protein is present in the urine of a subject. In human subjects, proteinuria is often diagnosed by urinanlysis. Clinically, proteinuria may be determined when there is presence of urinary protein in amounts exceeding 0.3 g in a 24-hour urine collection or in concentrations more than 1 g per liter (1+ to 2+ by standard turbidometric methods) in a random urine collection on two or more occasions at least 6 hours apart. "Proteinuria” is sometimes considered to be synonymous with "albuminuria”, although the latter refers specifically to presence of albumin protein in the urine, whereas proteinuria may encompass the presence of proteins other than albumin.
- the term "subject suspected of having diabetes” refers to a subject that presents one or more symptoms indicative of diabetes or a diabetes-related condition (e.g., diabetes mellitus type 1, diabetes mellitus type 2, gestational diabetes, pre-diabetes, metabolic syndrome, syndrome X) (e.g., polyuria, polydipsia, nocturia, fatigue, weight loss) or is being screened for diabetes ( e.g ., during a routine physical).
- a subject suspected of having diabetes or a diabetes-related condition may also have one or more risk factors.
- a subject suspected of having diabetes or a diabetes-related condition has generally not been tested for diabetes or a diabetes-related condition.
- a "subject suspected of having diabetes” encompasses an individual who has received a preliminary diagnosis (e.g ., a random plasma glucose level) but for whom a confirmatory test (e.g ., fasting glucose plasma level, hemoglobin HA1C, glucose tolerance test) has not been done or for whom the type of diabetes is not known.
- a confirmatory test e.g ., fasting glucose plasma level, hemoglobin HA1C, glucose tolerance test
- the term "subject diagnosed with diabetes” refers to a subject who has been tested and found to have diabetes or a diabetes-related condition (e.g., diabetes mellitus type 1, diabetes mellitus type 2, gestational diabetes, pre-diabetes, metabolic syndrome, syndrome X) (e.g., a random plasma glucose level of ⁇ 200 mg/dL or greater, a fasting glucose plasma level of ⁇ 110 mg/dL occurring on two separate occasions, or 2 hours post glucose load (75 g) plasma glucose of ⁇ 200 mg/dL on two separate occasions).
- a diabetes-related condition e.g., diabetes mellitus type 1, diabetes mellitus type 2, gestational diabetes, pre-diabetes, metabolic syndrome, syndrome X
- a random plasma glucose level of ⁇ 200 mg/dL or greater e.g., a fasting glucose plasma level of ⁇ 110 mg/dL occurring on two separate occasions, or 2 hours post glucose load (75 g) plasma glucose of ⁇ 200 mg/dL
- Diabetes may be diagnosed using any suitable method, including but not limited to, measurements of random plasma glucose level, fasting plasma glucose level, hemoglobin A1c (HbA 1c ) levels, glycosylated hemoglobin (GHb) levels.
- HbA 1c hemoglobin A1c
- GHb glycosylated hemoglobin
- initial diagnosis refers to a test result of initial diabetes diagnosis that reveals elevated plasma glucose levels (e.g ., random plasma glucose levels).
- the term "subject at risk for diabetes” refers to a subject with one or more risk factors for developing diabetes or a diabetes-related condition.
- Risk factors include, but are not limited to, obesity (particularly central or abdominal obesity), ethnicity, gender, age, genetic predisposition, diet, lifestyle (particularly sedentary lifestyle), and diseases or conditions that can lead to secondary diabetes (e.g., treatment with glucocorticoids, Cushing syndrome, acromegaly, pheochromocytoma, surgery, other endocrine disorders).
- characterizing diabetes in subject refers to the identification of one or more properties of diabetes disease or a diabetes-related disease in a subject, including but not limited to, plasma glucose levels (random, fasting, or upon glucose challenge); HbA 1c levels; glycosylated hemoglobin (GHb) levels; microalbumin levels or albumin-to-creatinine ratio (ACR); insulin levels; C-peptide levels; antibodies to insulin, islet cells, or glutamic acid decarboxylase (GAD); levels of anti-GAD65 antibody (e.g., as an indicator of latent autoimmune diabetes of adults).
- the term "providing a prognosis” refers to providing information regarding the impact of the presence of diabetes on a subject's future health (e.g., expected morbidity or mortality, the likelihood of getting diabetes, and the risk of diabetes-related complications).
- non-human animals refers to all non-human animals including, but not limited to, vertebrates such as rodents, non-human primates, ovines, bovines, ruminants, lagomorphs, porcines, caprines, equines, canines, felines, aves, etc.
- eukaryote refers to organisms distinguishable from “prokaryotes.” It is intended that the term encompass all organisms with cells that exhibit the usual characteristics of eukaryotes, such as the presence of a true nucleus bounded by a nuclear membrane, within which lie the chromosomes, the presence of membrane-bound organelles, and other characteristics commonly observed in eukaryotic organisms. Thus, the term includes but is not limited to such organisms as fungi, protozoa, and animals ( e.g., humans).
- in vitro refers to an artificial environment and to processes or reactions that occur within an artificial environment.
- in vitro environments can consist of, but are not limited to, test tubes and cell culture.
- in vivo refers to the natural environment (e.g., an animal or a cell) and to processes or reaction that occur within a natural environment.
- sample is used in its broadest sense. In one sense, it is meant to include a specimen or culture obtained from any source, as well as any biological. Biological samples may be obtained from animals (including humans) and encompass fluids, solids, tissues, and gases. Biological samples include blood products, such as plasma, serum and the like. Such examples are not however to be construed as limiting the sample types applicable to the present invention.
- an effective amount refers to the amount of a compound (e.g., a combination of an indoline and an anti-aldosterone compound as described herein) sufficient to effect beneficial or desired results.
- An effective amount can be administered in one or more administrations, applications or dosages and is not limited to or intended to be limited to a particular formulation or administration route.
- co-administration refers to the administration of at least two agent(s) (e.g., an indoline and an anti-aldosterone as described herein) or therapies to a subject.
- agent(s) e.g., an indoline and an anti-aldosterone as described herein
- the co-administration of two or more agents/therapies is concurrent.
- a first agent/therapy is administered prior to a second agent/therapy.
- formulations and/or routes of administration of the various agents/therapies used may vary.
- the appropriate dosage for co-administration can be readily determined by one skilled in the art.
- agents/therapies when agents/therapies are co-administered, the respective agents/therapies are administered at lower dosages than appropriate for their administration alone.
- co-administration is especially desirable in examples of the present disclosure where the co-administration of the agents/therapies lowers the requisite dosage of a known potentially harmful (e.g., toxic) agent(s).
- composition refers to the combination of an active agent with a carrier, inert or active, making the composition especially suitable for diagnostic or therapeutic use in vitro, in vivo or ex vivo.
- the term "pharmaceutically acceptable carrier” refers to any of the standard pharmaceutical carriers, such as a phosphate buffered saline solution, water, emulsions ( e.g., such as an oil/water or water/oil emulsions), and various types of wetting agents.
- the compositions also can include stabilizers and preservatives.
- stabilizers and adjuvants see e.g., Martin, Remington's Pharmaceutical Sciences, 15th Ed., Mack Publ. Co., Easton, PA (1975 ).
- the term "pharmaceutically acceptable salt” refers to any pharmaceutically acceptable salt (e.g., acid or base) of a compound of the present invention which, upon administration to a subject, is capable of providing a compound of this invention or an active metabolite or residue thereof.
- salts of the compounds of the present invention may be derived from inorganic or organic acids and bases.
- acids include, but are not limited to, hydrochloric, hydrobromic, sulfuric, nitric, perchloric, fumaric, maleic, phosphoric, glycolic, lactic, salicylic, succinic, toluene-p-sulfonic, tartaric, acetic, citric, methanesulfonic, ethanesulfonic, formic, benzoic, malonic, naphthalene-2-sulfonic, benzenesulfonic acid, and the like.
- Other acids such as oxalic, while not in themselves pharmaceutically acceptable, may be employed in the preparation of salts useful as intermediates in obtaining the compounds of the invention and their pharmaceutically acceptable acid addition salts.
- bases include, but are not limited to, alkali metals (e.g., sodium) hydroxides, alkaline earth metals (e.g., magnesium), hydroxides, ammonia, and compounds of formula NW 4 + , wherein W is C 1-4 alkyl, and the like.
- salts include, but are not limited to: acetate, adipate, alginate, aspartate, benzoate, benzenesulfonate, bisulfate, butyrate, citrate, camphorate, camphorsulfonate, cyclopentanepropionate, digluconate, dodecylsulfate, ethanesulfonate, fumarate, flucoheptanoate, glycerophosphate, hemisulfate, heptanoate, hexanoate, hydrochloride, hydrobromide, hydroiodide, 2-hydroxyethanesulfonate, lactate, maleate, methanesulfonate, 2-naphthalenesulfonate, nicotinate, oxalate, palmoate, pectinate, persulfate, phenylpropionate, picrate, pivalate, propionate, succinate, tartrate, thiocyanate,
- salts of the compounds of the present description are contemplated as being pharmaceutically acceptable.
- salts of acids and bases that are non-pharmaceutically acceptable may also find use, for example, in the preparation or purification of a pharmaceutically acceptable compound.
- the term "instructions for administering said compound to a subject,” and grammatical equivalents thereof, includes instructions for using the compositions contained in a kit for the treatment of proteinuria and/or hypertension (e.g., providing dosing, route of administration, decision trees for treating physicians for correlating patient-specific characteristics with therapeutic courses of action).
- the indoline and/or anti-aldosterone combination therapies of the present description can be packaged into a kit, which may include instructions for administering the compounds to a subject.
- the term "obesity” refers to the state of being in excess of one's ideal weight, wherein determination of ideal weight takes into account multiple factors including but not limited to one's height, age, sex, and build. In some examples of the present disclosure, “obese” is defined as having a body mass index (BMI) of 30 or greater.
- BMI body mass index
- body mass index As used herein, the term “body mass index” or “BMI” is defined as a person's weight in kilograms (kg) divided by their height in meters (m) squared. While BMI strongly correlates with overall fat content, one of ordinary skill in the art understands that some very muscular people may have a high BMI without undue health risks.
- diabetes refers to a metabolic or endocrinological disease, condition, or state affecting control of glycemia.
- Diabetes or diabetes-related conditions may affect sensitivity to insulin or production of insulin. Examples of diabetes or diabetes-related diseases or condition include but are not limited to impaired insulin signaling, diabetes mellitus, type I diabetes, type II diabetes, gestational diabetes, metabolic syndrome, metabolic syndrome X, syndrome X, insulin resistance syndrome, Reaven's syndrome, CHAOS, and malnutrition-related diabetes mellitus.
- edema refers to an abnormal accumulation of fluid beneath the skin, or in one or more cavities of the body.
- causes of edema which are generalized to the whole body can cause edema in multiple organs and peripherally.
- severe heart failure e.g., congestive heart failure
- pulmonary edema e.g., pleural effusions
- ascites and peripheral edema the last of which effects can also derive from less serious causes.
- Organ-specific edema types include cerebral edema, pulmonary edema, pleural efflusions, corneal edema, periorbital edema, cutaneous edema, myxedema, edema of the feet, and lymphedema.
- the term "congestive heart failure” refers to an imbalance in pump function in which the heart fails to adequately maintain the circulation of blood.
- CHF New York Heart Association's functional classification of CHF, Class I describes a patient whose normal physical activity is not limited by symptoms. Class II occurs when ordinary physical activity results in fatigue, dyspnea, or other symptoms. Class III is characterized by a marked limitation in normal physical activity. Class IV is defined by symptoms at rest or with any physical activity.
- indoline refers to compounds comprising an indoline moiety, particularly those having diuretic and/or anti-hypertensive function.
- examples of indulines include but are not limited to 1-[(tert-butylimino)methyl]-2-(3-indolyl) indoline HCl and derivatives thereof; 1-hydroxyalkanamine pyrano(3,4-B) indole derivatives (see, e.g., PCT App. No.
- indoline compounds are described as compounds of formula I in which R1 is lower alkyl; R2 is hydrogen or lower alkyl; R3 and R4 each independently is hydrogen, lower alkyl halo, nitro, trifluoromethyl or lower alkoxy; R5 and R6 each independently is hydrogen or lower alkyl or R5 and R6 together with the nitrogen atom form a pyrrol-1-yl, piperidino or morpholino ring; R7 is hydrogen or lower alkyl; Alk1 and Alk2 each independently is a straight or branched chain lower alkylene having one to six carbon atoms; and X is oxa or thia, and therapeutically acceptable acid addition salts thereof.
- the above compounds are diuretic agents, which also possess anti-hypertensive activity. They may be used alone or with other diuretic agents. Pharmaceutical compositions containing the compounds and processes for preparing the compounds are also described.
- anti-aldosterone agent or “aldosterone antagonist” refers to an agent that antagonizes an effect or function (e.g., a physiological effect or function, a biochemical effect or function, a molecular effect or function) of aldosterone.
- Anti-aldosterone agents alsoinclude but are not limited to spironolatone, eplerenone, canrenone, anti-aldosterone antibodies, potassium canrenoate, carbolactones such as spirorenone, progestin analogs such as drospirenone, mesperinone and combined B-Type Natriuretic Peptide and Vasopressin-2 Receptor antagonism with Tolvaptan.
- the present description relates to methods, compositions, and kits for the treatment of subjects at risk for or suffering from proteinuria and hypertension (e.g., proteinuria and/or hypertension arising from primary renal disease (e.g., focal segmental glomerulosclerosis, glomerular disease) or secondary to other conditions (e.g., diabetes, diabetic nepropathy, cirrhosis, liver disease).
- proteinuria and hypertension e.g., proteinuria and/or hypertension arising from primary renal disease (e.g., focal segmental glomerulosclerosis, glomerular disease) or secondary to other conditions (e.g., diabetes, diabetic nepropathy, cirrhosis, liver disease).
- an indoline e.g., indapamide
- an anti-aldosterone agent e.g., spironolactone and/or eplerenone
- Proteinuria is caused by many diseases and conditions, as detailed below. Urinary protein loss is a frequent hallmark of the development and progression of diabetic nephropathy, a major source of morbidity for diabetic patients. Optimal control of blood pressure retards the progression of diabetic nephropathy, but in most cases, requires multiple medications that provide additive benefits via different mechanisms. Investigations conducted during the course of developing some examples of the present disclosure of the present description identified combination therapies providing renoprotection, e.g., by preventing or treating proteinuria.
- combination therapies comprising an indoline agent (e.g., indapamide) plus an anti-aldosterone agent (e.g., spironolactone, eplerenone) provide superior lowering of proteinuria (e.g., albuminuria) in comparison to, e.g., traditional thiazide diuretics.
- an indoline agent e.g., indapamide
- an anti-aldosterone agent e.g., spironolactone, eplerenone
- proteinuria e.g., albuminuria
- renoprotective effects occur independently of blood pressure changes, either when combination therapy examples of the present disclosure of the present invention are administered alone or when they are added to other therapies (e.g., added to first-line drugs that block the renin-angiotensin-aldosterone system).
- Combination therapy, composition, and method examples of the present disclosure of the present description provide numerous unexpected benefits over existing therapies and over the administration of single agents (e.g., a single indoline agent, a single anti-aldosterone agent).
- combination therapies of the present description markedly reduce proteinuria.
- combination therapies of the present description provide synergistic effects in proteinuria reduction as compared to administration of either agent alone (e.g., a single indoline agent, a single anti-aldosterone agent).
- combination therapies of the present description provide increased reduction in proteinuria in comparison to other combinations (e.g., an angiotensin-converting enzyme inhibitor (ACE inhibitor) in combination with an angiotensin receptor blocker (ARB); an ACE inhibitor and a diuretic; an ARB and a diuretic; an ACE inhibitor and an anti-aldosterone agent (e.g., spironolactone); an ARB and an anti-aldosterone agent (e.g., spironolactone); an ACE inhibitor and a calcium channel blocker; an ACE inhibitor and a beta blocker; an ARB and a beta blocker).
- ACE inhibitor an angiotensin-converting enzyme inhibitor
- ARB an ACE inhibitor and a diuretic
- an ACE inhibitor and an anti-aldosterone agent e.g., spironolactone
- an ARB and an anti-aldosterone agent e.g., spironolactone
- combination therapies of the present description result in fewer undesirable side effects as compared to side effects occurring when either single agent is administered alone (e.g., a single indoline agent, a single anti-aldosterone agent), such side effects including but not limited to effects on cardiac ion channels, effects on serum potassium levels, effects on serum magnesium levels, effects on serum uric acid levels.
- single agent e.g., a single indoline agent, a single anti-aldosterone agent
- side effects including but not limited to effects on cardiac ion channels, effects on serum potassium levels, effects on serum magnesium levels, effects on serum uric acid levels.
- aldosterone escape occurs despite treatment with ACE inhibitors and ARBs, alone or in combination, irrespective of doses used.
- the mechanism of aldosterone escape is unknown, but could be related to inadequate ACE inhibition and the existence of multiple pathways for aldosterone release.
- combination therapies of the present description provide inhibition of the renin-angiotensin-aldosterone system without triggering aldosterone escape or angiotensin reactivation.
- Combination therapy, composition, and method examples of the present disclosure of the present description further provide benefits for reducing the risk of drug-induced cardiac arrhythmia (e.g., Torsade de Pointes, as described below).
- drug-induced cardiac arrhythmia e.g., Torsade de Pointes, as described below.
- indapamide causes an increased incidence in a form of tachyarrhythmia associated with long QT interval known as Torsade de Pointes (TdP).
- TdP Torsade de Pointes
- aldosterone antagonists accelerate repolarization, shorten QT interval and thereby reduce the risk of TdP by major effects on inhibition of inward Na + and Ca +2 currents.
- Proteinuria refers to the presence of an excess of serum proteins in the urine. There are three main mechanisms thought to cause proteinuria: 1) glomerular disease; 2) overflow proteinuria due to increased quantity of proteins in serum; and 3) low reabsorbtion at proximal tubule (fanconi). Proteinuria is often diagnosed by a simple dipstick test, although if urine is dilute, it is possible for the test to give a false negative even with nephrotic range proteinuria. False negatives may also occur if the protein in the urine is composed mainly of globulins or Bence-Jones Proteins because the reagent on the test strips, Bromphenol blue, is highly specific for albumin.
- dipstick protein tests are quantified by measuring the total quantity of protein in a 24-hour urine collection test, and abnormal globulins by specific requests for protein electrophoresis.
- concentration of protein in the urine may be compared to the creatinine level in a spot urine sample. This is termed Protein/Creatinine Ratio (PCR).
- Proteinuria may be defined as a Protein:creatinine ratio >45 mg/mmol (which is equivalent to Albumin:creatinine ratio of >30 mg/mmol) with very high levels of nephrotic syndrome being for PCR > 100 mg/mmol.
- Proteinuria may be a sign of renal (kidney) damage. Since serum proteins are readily reabsorbed from urine, the presence of excess protein indicates either an insufficiency of absorption or impaired filtration. Diabetics may suffer from damaged nephrons and develop proteinuria. The most common cause of proteinuria in the United States is diabetes, and in any person with proteinuria and diabetes the etiology of the underlying proteinuria should be separated into two categories: diabetic proteinuria versus a category other than diabetic proteinuria.
- Symptoms of diminished oncotic pressure may include ascites, edema, and hydrothorax.
- Proteinuria of glomerular origin is a manifestation of generalized vascular disease and is therefore associated with adverse cardiovascular outcomes.
- Experimental and clinical evidence supports the association between severity of proteinuria and accelerated progression of chronic kidney disease and resulting renal failure. Leakage of protein across glomerular capillary basement membrane into the urinary space is followed by uptake of protein by the renal tubular epithelial cell, release of cytokines such as monocyte chemoattractant protein-1 and RANTES, resultant inflammation in renal tubulointerstitium, progressive fibrosis and thereby accelerated progression of renal disease.
- cytokines such as monocyte chemoattractant protein-1 and RANTES
- complement anaphylotoxin C3a is an important mediator of proteniuric glomerular and tubulointerstitial injury and can induce transition of renal tubular epithelial cells from an epithelial phenotype to phenotypic and functional characteristics of mesenchymal cells.
- Proteinuria may be a feature of conditions including but not limited to: nephrotic syndromes (i.e. intrinsic renal failure); pre-eclampsia; eclampsia; toxic kidney lesions; collagen vascular diseases (e.g. systemic lupus erythematosus); dehydration; glomerular diseases such as membranous glomerulonephritis, focal segmental glomerulonephritis, and minimal change disease (lipoid nephrosis); strenuous exercise; stress; benign orthostatic (postural) proteinuria; focal segmental glomerulosclerosis (FSGS); IgA nephropathy (i.e.
- IgM nephropathy membranoproliferative glomerulonephritis; membranous nephropathy; sarcoidosis; Alport's syndrome; diabetes mellitus; drugs (e.g. NSAIDs, nicotine, penicillamine, gold and other heavy metals, ACE inhibitors, antibiotics, opiates especially heroin); Fabry's disease; infections (e.g.
- HIV syphilis, hepatitis, post-streptococcal infection
- aminoaciduria Fanconi syndrome,;hypertensive nephrosclerosis; interstitial nephritis; sickle cell disease; hemoglobinuria; multiple myeloma; organ rejection; Ebola hemorrhagic fever; Nail Patella Syndrome; Familial Mediterranean fever; HELLP Syndrome; Wegener's Granulomatosis; and Glycogen Storage Disease Type 1.
- Indapamide is a diuretic with a unique structure that is distinct from diuretics belonging to the class of thiazides, loop diuretics, carbonic anhydrase inhibitors and potassium sparing diuretics such as triamterene, amiloride or aldosterone receptor antagonists such as spironolactone and eplerenone.
- the US trade name for indapamide is Lozol.
- Indapamide is marketed as Natrilix outside of the US.
- Indapamide is in a class of antihypertensive/diuretics, the indolines. Its molecule contains both a polar sulfamoyl chlorobenzamide moiety and a lipid-soluble methylindoline moiety.
- indapamide 4-Chloro-N- (2-methyl-lindolinyl) -3-Sulfamoylbenzamide.
- Indapamide resembles thiazide diuretics in renal actions, in that both agents inhibit sodium and chloride reabsorption in the distal tubule. Consequently, indapamide exhibits diuretic properties similar to thiazide diuretics. Furthermore, like thiazides, indapamide administration is associated with hypokalemia, hyponatremia, hypercalcemia and hyperuricemia.
- indapamide confers marked differences in extra-renal actions, compared with thiazides, such effects including but not limited to: calcium channel antagonistic activity; blockage of the tissue rennin-angiotensin system; inhibition of the adrenerginc system thereby lowering plasma catchecholamine levels; and improvement in vascular reactivity by enhancement of endothelium-dependent vascular relaxation (in contrast to thiazides, which impair vascular reactivity by inhibition of endothelium-dependent vascular relaxation).
- indapamide confers several advantages over thiazide diuretics, such advantages including but not limited to antihypertensive action manifest in the absence of renal function, as in anuric patients on dialysis; a lack of undesirable decrease in glomerular filtration rate (GFR) and renal plasma flow (in contrast to thiazide durietics); reduction of proteinuria effectively in proteinuric states independent of anti-hypertensive action; and absence of increased risk of metabolic syndrome ( Ames et al. (1996) Am. J. Cardiol. 77:12B-16B ; herein incorporated by reference in its entirety) in contrast to thiazides, which can increase risk of metabolic syndrome; and utility even when GFR is lower than 30 ml/min.
- Spironolactone is a competitive antagonist of the aldosterone-sensitive sodium channel in the distal cortical tubule ( Horisberger et al. (1987) Ren. Physiol. 10:198-220 ; herein incorporated by reference in its entirety). Because of its natriuretic properties, spironolactone is an effective anti-hypertensive agent that provides additive effects when used in combination with other anti-hypertensive agents, including ACEI or ARB agents. Spironolactone is uniquely effective for offsetting the hypokalemia typically associated with other diuretics, and may be particularly efficacious for states of hyperaldosteronism ( Lim et al. (2001) J. Hypertens.
- spironolactone was speculated to substantially reduce albuminuria and retard the progression of diabetic nephropathy in a significant proportion of patients who were not receiving the maximum possible protection from their ACEI or ARB agent.
- the effect of addition of spironolactone to existing ACEI or ARB treatment was unknown, especially with regard to possible adverse effects on potassium levels and GFR.
- Additional anti-aldosterone agents include but are not limited to eplerenone, canrenone, anti-aldosterone antibodies, potassium canrenoate, carbolactones such as spirorenone, progestin analogs such as drospirenone, mesperinone and combined B-Type Natriuretic Peptide and Vasopressin-2 Receptor antagonism with Tolvaptan.
- Torsade de pointes is a distinctive form of polymorphic ventricular tachycardia (VT) characterized by a gradual change in the amplitude and twisting of the QRS complexes around the isoelectric line.
- Torsade de pointes (torsade) is associated with a prolonged QT interval, which may be congenital or acquired. It usually terminates spontaneously but frequently recurs and may degenerate into sustained VT and ventricular fibrillation.
- Torsade is defined as a polymorphous VT in which the morphology of the QRS complexes varies from beat to beat.
- the ventricular rate can range from 150 beats per minute (bpm) to 250 bpm.
- the original report described regular variation of the morphology of the QRS vector from positive to net negative and back again. This was symbolically termed torsade de pointes, or "twisting of the point" about the isoelectric axis, because it reminded the original authors of the torsade de pointes movement in ballet. Most cases exhibit polymorphism, but the axis changes may not have regularity.
- the definition also requires that the QT interval be increased markedly (usually to 600 msec or greater). Cases of polymorphous VT, which are not associated with a prolonged QT interval, are treated as generic VT. Torsade usually occurs in bursts that are not sustained; thus, the rhythm strip usually shows the patient's baseline QT prolongation.
- the underlying basis for rhythm disturbance is delay in phase III of the action potential.
- the delay is mediated by the hERG potassium channel. This prolonged period of repolarization and the inhomogeneity of repolarization times among myocardial fibers allow the dysrhythmia to emerge.
- the initiating electrophysiologic mechanism may be triggered activity or reentry.
- Genotypes LQT1 and LQT2 have slow potassium channels, while LQT3 shows defects in the sodium channels. Treatment modalities soon may be based on the genotype of the individual.
- Torsade is a life-threatening arrhythmia and may present as sudden cardiac death in patients with structurally normal hearts.
- the corrected QT interval is longer in persons of European descent than in persons of African descent, thus explaining the lower susceptibility to acquired torsade in persons of African descent.
- Females are more prone to the development of torsade than males because they have longer QT intervals.
- Torsade occurs in patients of a wide age range, from newborn to 86 years. If it occurs at an early age, the cause usually is due to congenital long QT syndrome. In later years, the cause usually is due to acquired long QT syndrome.
- Patients with torsade usually present with recurrent episodes of palpitations, dizziness, and syncope; however, sudden cardiac death can occur with the first episode.
- Nausea, cold sweats, shortness of breath, and chest pain also may occur but are nonspecific and can be produced by any form of tachyarrhythmia.
- Indapamide is known to be associated with highest risk of TdP ( Sander, Guillory et al. (2002) Am. J. Geriatr. Cardiol. 11:197-202 ; herein incorporated by reference in its entirety).
- Table 1 Action of indapamide and anti-aldosterone agent on mechanisms underlying ventricular repolarization, QT interval and Torsade Electrophysiology of heart Effect on Effect on QT interval Aldosterone Anti-aldosterone Indapamide Inward sodium current Slows repolarization Prolongs QT Increases sodium current (Boixel, Gaviltet et al.
- Indapamide has been shown to produce QT interval prolongation and torsade de pointes (TdP) in the presence of normal electrolytes ( Letsas, Alexanian et al. (2006) Int. J. Cardiol. 112:373-374 ; herein incorporated by reference in its entirety).
- the major action of indapamide that leads to slowing of repolarization, prolongation of QT interval and thereby predisposition to TdP is a direct electrophysiological effect on ionic currents.
- indapamide blocks the slow component of the delayed rectifier K+ current (IKs) ( Turgeon, Daleau et al. (1994) Circ. Res. 75:879-886 ; herein incorporated by reference in its entirety).
- the present description finds use in the treatment of subjects with diabetes or a diabetes-related condition involving e.g., impaired glucose tolerance, impaired insulin sensitivity, impaired insulin production.
- diabetes-related condition involving e.g., impaired glucose tolerance, impaired insulin sensitivity, impaired insulin production.
- Such conditions and disease states include diabetes mellitus, type I diabetes, type II diabetes, gestational diabetes, metabolic syndrome, metabolic syndrome X, syndrome X, insulin resistance syndrome, Reaven's syndrome, CHAOS, and malnutrition-related diabetes mellitus.
- Such patients are at risk for and/or experience an increased incidence and severity of renal dysfunction and renal disease, as described below.
- Diabetic nephropathy also known as Kimmelstiel-Wilson syndrome and intercapillary glomerulonephritis
- Diabetic nephropathy is a progressive kidney disease caused by angiopathy of capillaries in the kidney glomeruli. It is characterized by nephrotic syndrome and diffuse glomerulosclerosis. It is due to longstanding diabetes mellitus, and is a prime indication for dialysis in many Western countries.
- Diabetic nephropathy is the most common cause of chronic kidney failure and end-stage kidney disease in the United States. People with both type 1 and type 2 diabetes are at risk. The risk is higher if blood-glucose levels are poorly controlled. Further, once nephropathy develops, the greatest rate of progression is seen in patients with poor control of their blood pressure. Patients with high cholesterol level in their blood are also at greater risk.
- the earliest detectable change in the course of diabetic nephropathy is a thickening in the glomerulus.
- the kidney may start producing more serum albumin (plasma protein) than normal in the urine (albuminuria), referred to as "microalbuminuria”.
- plasma protein serum albumin
- microalbuminuria serum albuminuria
- the amounts of albumin excreted in the urine increases, and may be detected by ordinary urinalysis techniques.
- a kidney biopsy shows diabetic nephropathy.
- diabetic nephropathy has no symptoms. Symptoms develop in later stages and may be a result of excretion of high amounts of protein in the urine or due to renal failure. Symptoms include but are not limited to edema, anorexia, nausea, vomiting, malaise, fatigue, headache, frequent hiccups, and generalized itching.
- the first laboratory abnormality is a positive microalbuminuria test. Most often, the diagnosis is suspected when a routine urinalysis shows proteinuria. The urinalysis may also show glucose in the urine, especially if blood glucose is poorly controlled. Serum creatinine and BUN may increase as kidney damage progresses.
- a kidney biopsy confirms the diagnosis, although it is not always necessary if the case is straightforward, with a documented progression of proteinuria over time and presence of diabetic retinopathy on examination of the retina of the eyes.
- Standard treatments include administration of ACE inhibitor agents and/or ARB agents; however, combination therapy, according to the ONTARGET study ( Yusuf et al. (2008) New Engl. J. Med. 358:1547-1559 ; herein incorporated by reference in its entirety) can worsen major renal outcomes including increasing serum creatinine and causing a greater demand in estimated GFR.
- Diabetic nephropathy continues to gradually progress. Complications of chronic kidney failure are more likely to occur earlier, and progress more rapidly, when it is caused by diabetes than when it occurs due to other causes. Even after initiation of dialysis or after transplantation, people with diabetes tend to do worse than those without diabetes. Possible complications include but are not limited to hypoglycemia, rapidly progressing chronic kidney failure, end-stage kidney disease, hyperkalemia, severe hypertension, complications of hemodialysis, complications of kidney transplant, coexistence of other diabetes complications, peritonitis (if peritoneal dialysis is used), and increased infections.
- liver failure is the inability of the liver to perform its normal synthetic and metabolic function as part of normal physiology.
- Two forms include acute liver failure, and chronic liver failure.
- acute liver failure hepatic encephalopathy (confusion, stupor and coma) occurs within four weeks of the first symptoms of a liver problem (such as jaundice).
- Chronic liver failure usually occurs in the context of cirrhosis (itself caused by factors including but not limited to excessive alcohol intake, hepatitis B, hepatitis C, or autoimmune, hereditary and metabolic causes (e.g., iron or copper overload or non-alcoholic fatty liver disease).
- Hypertension is a chronic medical condition in which the blood pressure is elevated. It is also referred to as high blood pressure or shortened to HT, HTN or HPN.
- hypertension normally refers to systemic, arterial hypertension. Hypertension can be classified as either essential (primary) or secondary. Essential or primary hypertension indicates that no medical cause is known. Secondary hypertension indicates that the high blood pressure is a result of another condition, such as kidney disease or tumors (e.g., adrenal adenoma or pheochromocytoma).
- a 2003 American Heart Association classification recommends blood pressure criteria for defining normal blood pressure, prehypertension, hypertension (stages I and II), and isolated systolic hypertension, the latter being common occurrence among the elderly. These readings are based on the average of seated blood pressure readings that were properly measured during two or more office visits. In individuals older than 50 years, hypertension is considered to be present when a person's blood pressure is consistently at least 140 mmHg systolic or 90 mmHg diastolic.
- Various agents find use in controlling hypertension (systolic and/or diastolic hypertension); e.g., indapamide is efficacious for systolic hypertension.
- CHF congestive heart failure
- pulmonary edema congestive heart failure
- CHF is an imbalance in pump function in which the heart fails to adequately maintain the circulation of blood.
- CHF can be categorized as right sided and left sided ventricular failure.
- Right-sided failure causes elevated systemic venous pressure
- left ventricular failure is secondary to reduced forward flow into the aorta and systemic circulation.
- heart failure can be subdivided into systolic and diastolic dysfunction.
- Systolic dysfunction is characterized by a dilated left ventricle with impaired contractility, whereas diastolic dysfunction occurs in a normal or intact left ventricle with impaired ability to relax and receive as well as eject blood.
- Class I describes a patient whose normal physical activity is not limited by symptoms.
- Class II occurs when ordinary physical activity results in fatigue, dyspnea, or other symptoms.
- Class III is characterized by a marked limitation in normal physical activity.
- Class IV is defined by symptoms at rest or with any physical activity.
- CHF and/or pulmonary edema may be caused by coronary artery disease (e.g., secondary to loss of left ventricular muscle), ongoing ischemia, decreased diastolic ventricular compliance, hypertension, valvular heart disease, congenital heart disease, other cardiomyopathies, myocarditis, infectious endocarditis, pregnancy, and hyperthyroidism.
- CHF is often precipitated by cardiac ischemia or dysrhythmias, cardiac or extracardiac infection, pulmonary embolus, physical or environmental stresses, changes or noncompliance with medical therapy, dietary indiscretion, or iatrogenic volume overload.
- methods of the present description find use in the treatment of edema, which is an abnormal accumulation of fluid beneath the skin, or in one or more cavities of the body.
- edema which is an abnormal accumulation of fluid beneath the skin, or in one or more cavities of the body.
- causes of edema which are generalized to the whole body can cause edema in multiple organs and peripherally.
- severe heart failure CHF, as described supra
- pulmonary edema pulmonary edema
- pleural effusions ascites and peripheral edema
- Organ-specific edema types include cerebral edema, pulmonary edema, pleural efflusions, corneal edema, periorbital edema, cutaneous edema, myxedema, edema of the feet, and lymphedema.
- Kidney Diseases (Nephropathy)
- Glomerular diseases include many conditions with a variety of genetic and environmental causes, but they fall into two major categories: glomerulonephritis, wherein there is inflammation of the membrane tissue in the kidney that serves as a filter, separating wastes and extra fluid from the blood; and glomerulosclerosis, wherein there is scarring or hardening of the tiny blood vessels within the kidney. Although glomerulonephritis and glomerulosclerosis have different causes, they can both lead to kidney failure.
- Types of nephropathies include but are not limited to drug-induced nephropathy, Systemic lupus erythematosus, Goodpasture's syndrome, IgA nephropathy, Alport syndrome, acute post-streptococcal glomerulonephritis (PSGN), bacterial endocarditis, HIV-induced nephropathy, glomerulosclerosis, diabetic nephropathy, focal segmental glomerulosclerosis (FSGS), membranous nephropathy (also called membranous glomerulopathy), and minimal change disease (MCD).
- PSGN acute post-streptococcal glomerulonephritis
- bacterial endocarditis HIV-induced nephropathy, glomerulosclerosis, diabetic nephropathy, focal segmental glomerulosclerosis (FSGS), membranous nephropathy (also called membranous glomerulopathy), and minimal change disease (MCD).
- Stages of kidney failure are categorized as acute renal failure, chronic kidney disease, and total kidney failure (sometimes called end-stage renal disease or ESRD).
- compositions and methods of the present description provide means of ameliorating this problem by effectively administering a combined therapy approach.
- traditional combination therapy may be employed in combination with the compositions of the present description.
- combination therapies comprising an indoline agent and an anti-aldosterone agent may be used before, after, or in combination with traditional therapies.
- compositions described herein and at least one other agent are provided in a combined amount effective to have a therapeutic effect the cell.
- This process may involve contacting the cells with multiple agent(s) or factor(s) at the same time. This may be achieved by contacting the cell with a single composition or pharmacological formulation that includes both agents, or by contacting the cell with two distinct compositions or formulations, at the same time, wherein one composition includes, for example, an expression construct and the other includes a therapeutic agent.
- indoline (e.g., indapamide) treatment may precede or follow the second agent (e.g., an anti-aldosterone agent) by intervals ranging from minutes to weeks.
- second agent e.g., an anti-aldosterone agent
- indoline agent e.g., indapamide
- anti-aldosterone agent e.g., an anti-aldosterone agent
- cells are contacted with both modalities within about 12-24 hours of each other and, more preferably, within about 6-12 hours of each other, with a delay time of only about 12 hours being most preferred. In some situations, it may be desirable to extend the time period for treatment significantly, however, where several days (2 to 7) to several weeks (1 to 8) lapse between the respective administrations.
- indoline agent e.g., indapamide
- anti-aldosterone agent e.g., spironolactone
- both agents are delivered to a cell in a combined amount effective to promote desired therapeutic outcome (e.g., decreased proteinuria, lowered blood pressure).
- one or more compounds of the description and an additional active agent are administered to a subject, more typically a human, in a sequence and within a time interval such that the compound can act together with the other agent to provide an enhanced benefit relative to the benefits obtained if they were administered otherwise.
- the additional active agents can be co-administered by co-formulation, administered at the same time or administered sequentially in any order at different points in time; however, if not administered at the same time, they should be administered sufficiently close in time so as to provide the desired therapeutic or prophylactic effect.
- the compound and the additional active agents exert their effects at times which overlap.
- Each additional active agent can be administered separately, in any appropriate form and by any suitable route.
- the compound is administered before, concurrently or after administration of the additional active agents.
- the compound and the additional active agents are administered less than about 1 hour apart, at about 1 hour apart, at about 1 hour to about 2 hours apart, at about 2 hours to about 3 hours apart, at about 3 hours to about 4 hours apart, at about 4 hours to about 5 hours apart, at about 5 hours to about 6 hours apart, at about 6 hours to about 7 hours apart, at about 7 hours to about 8 hours apart, at about 8 hours to about 9 hours apart, at about 9 hours to about 10 hours apart, at about 10 hours to about 11 hours apart, at about 11 hours to about 12 hours apart, no more than 24 hours apart or no more than 48 hours apart.
- the compound and the additional active agents are administered concurrently.
- the compound and the additional active agents are administered concurrently by co-formulation.
- the compound and the additional active agents are administered at about 2 to 4 days apart, at about 4 to 6 days apart, at about 1 week part, at about 1 to 2 weeks apart, or more than 2 weeks apart.
- indoline agent e.g., indapamide
- an anti-aldosterone agent and optionally additional active agents
- Cycling therapy involves the administration of a first agent for a period of time, followed by the administration of a second agent and/or third agent for a period of time and repeating this sequential administration. Cycling therapy can provide a variety of benefits, e.g., reduce the development of resistance to one or more of the therapies, avoid or reduce the side effects of one or more of the therapies, and/or improve the efficacy of the treatment.
- one or more compounds of some examples of the present disclosure of the present description and optionally an additional active agent are administered in a cycle of less than about 3 weeks, about once every two weeks, about once every 10 days or about once every week.
- One cycle can comprise the administration of a first active agent and optionally the second active agent by infusion over about 90 minutes every cycle, about 1 hour every cycle, about 45 minutes every cycle, about 30 minutes every cycle or about 15 minutes every cycle.
- Each cycle can comprise at least 1 week of rest, at least 2 weeks of rest, at least 3 weeks of rest.
- the number of cycles administered is from about 1 to about 12 cycles, more typically from about 2 to about 10 cycles, and more typically from about 2 to about 8 cycles.
- Courses of treatment can be administered concurrently to a subject, i.e., individual doses of the additional active agents are administered separately yet within a time interval such that the inventive compound can work together with the additional active agents.
- one component can be administered once per week in combination with the other components that can be administered once every two weeks or once every three weeks.
- the dosing regimens are carried out concurrently even if the therapeutics are not administered simultaneously or during the same day.
- indoline agent e.g., indapamide
- anti-aldosterone agent e.g., spironolactone
- Tables 2 Some examples of the present disclosure of combination therapy dosage forms are illustrated in Tables 2.
- combinations of anti-aldosterone agents with up to 1.25 mg of indapamide are primarily indicated for the treatment of particular disease states and/or conditions including but not limited to hypertension without significant renal disease or heart failure; ascites associated with liver failure; and/or mild heart failure.
- combinations of anti-aldosterone agents with 2.5-5 mg indapamide are used for treatment of diseases and/or conditions including but not limited to edema or hypertension associated with stage 3-5 chronic kidney disease, and/or edema or hypertension associated with moderate or severe heart failure.
- Table 2 Exemplary dosages of spironolactone or eplerenone in combination with exemplary doses of indapamide.
- Spironolactone or Eplerenone (mg) Indapamide (mg) 0.5 12.5 or 0.625 25 or 1.0 37.5 or 1.25 50 or 1.5 75 or 2.0 100 2.5 3.0
- the patient was treated with 100 mg losartan, metoprolol 75 mg and amlodipine 10 mg daily.
- the patient was treated with a combination of 25 mg spironolactone and 1.25 mg indapamide with a decline in albuminuria to 930 mg albumin per 1 gram of creatinine, a reduction of 48%.
- Baseline urinary albumin was 8 grams per 1 gram of creatinine, while the patient was being treated with 100 mg losartan daily.
- the patient was treated with 20 mg benazapril and 240 mg extended release diltiazem daily.
- the patient was treated with a combination of 25 mg spironolactone and 0.625 mg indapamide and albuminuria decreased to 82 mg albumin per 1 gram of creatinine, a reduction of 80%.
- a 44 year old Hispanic male with alcoholic liver disease was on long-standing treatment with 200 mg spironolactone daily.
- the patient presented with hypertension and chronic proteinuric and hematuric kidney disease secondary to chronic glomerulonephritis, likely IgA nephropathy.
- the patient had albuminuria of 2606 mg per 1 gram creatinine.
- For hypertension and edema 2.5 mg indapamide daily was started.
- albuminuria had decreased to 1081 mg per 1 gram of creatinine, a reduction of 58.5%, even though the patient had a blood pressure of 160/100 mm of Hg.
- a 64-year-old Hispanic female with diabetic nephropathy had 1346 mg albuminuria per gram creatinine while taking lisinopril 40 mg, verapamil ER 240 mg and indapamide 0.625 mg.
- Spironolactone 25 mg was added and within 2 months, her albuminuria decreased to 258 mg per gram creatinine, a reduction of 81%.
- metolazone and indapamide Two thiazide-like diuretics that are effective in patients with stage 4-5 chronic kidney disease are metolazone and indapamide.
- indapamide in combination with spironolactone but not metolazone in combination with spironolactone, was capable of reducing proteinuria.
- the following case study demonstrates the failure of cotherapy with metolazone and spironolactone to reduce proteinuria.
- the urine albumin/creatinine ratio at conclusion of treatment was 4.3.
- Patient had a pulse rate of 95 per minute, blood pressure 142/82 mm of Hg, body weight 74.4 kg, and pedal edema. Nifedipine and hydrochlorthiazide were discontinued. Patient was started on indapamide 2.5 mg every morning, losartan 50 mg daily and terazosin 2 mg at bedtime.
- Blood pressure was 168/108 mm Hg. Atenolol was discontinued. Patient was started on long acting diltiazem 300 mg daily, losartan was increased to 100 mg daily and 1.25 mg indapamide daily was added.
- Case 3 A 60 year old Hispanic male presenting with diabetic nephropathy, hypertension and estimated GFR of 27 ml/min had asymptomatic hyperuricemia with a baseline serum uric acid level of 10.3 mg/dL. The patient was being treated with losartan 100 mg per day for hypertension and proteinuria. The patient was started on indapamide 1.25 mg and spironolactone 25 mg per day for optimal control of blood pressure. After 3 months, serum uric acid ranged between 6.4-7.2 mg/dL, a decline of 30% to 38%.
- Case 4 A 56 year old Hispanic female with diabetic nephropathy, hypertension and bifascicular block presented with following baseline serum values: uric acid 7.5 mg/dL, creatinine 1.4 mg/dL, SUN 36 mg/dL, urine albumin to creatinine ratio 1015 mg/g.
- Patient was being treated with losartan 100 mg and amlodipine 5 mg per day for hypertension and proteinuria.
- Patient was started on Indapamide 1.25 mg per day for hypertension at time 0. After 9 months of treatment, serum creatinine and urea nitrogen were unchanged and serum uric acid was 7.0 mg/dL.
- a 6-month, prospective, open-label, randomized pilot study is described to compare the efficacy of the indapamide-spironolactone combination versus hydrochlorothiazide (HCTZ), when added to angiotensin-converting enzyme inhibitor (ACEI) or angiotensin receptor blocker (ARB) therapy, for reducing proteinuria while targeting a uniform blood pressure (BP) goal, across a wide spectrum of diabetic subjects with confirmed micro- or macroalbuminuria.
- Subjects will be recruited from the Diabetes and Nephrology specialty clinics at the Martin Luther King Jr. - Multi-Service Ambulatory Clinic in South Los Angeles, CA, USA.
- MLK-MACC serves a large community of low-income and low-educational level individuals in the inner city of South Los Angeles, consisting of approximately 70% Hispanic and 25% African-Americans. Male or female adult subjects with type 1 or type 2 diabetes and confirmed evidence of micro- or macroalbuminuria (30 mg per g urine creatinine or higher on at least two consecutive determinations), who are already being treated with an ACE inhibitor or ARB agent, will be enrolled.
- Baseline Assessment Screening will include a medical history, vital signs and anthropometry, CBC, complete chemistry panel (including electrolytes, BUN, serum creatinine, estimated GFR based on the MDRD equation and serum cystatin C, hepatic transaminases, calcium, uric acid), HbA 1c , fasting lipid profile, routine urinalysis, and a determination of urinary albumin-creatinine ratio (ACR) based on a spot urine sample. Subjects determined to be eligible based on this screening should have a repeat ACR performed within 1 week (or previously had an ACR determination performed within the past 6 months) for confirmation.
- complete chemistry panel including electrolytes, BUN, serum creatinine, estimated GFR based on the MDRD equation and serum cystatin C, hepatic transaminases, calcium, uric acid
- HbA 1c fasting lipid profile
- routine urinalysis routine urinalysis
- ACR urinary albumin-creatinine ratio
- Run-In Phase To minimize the potential influence that severe hyperglycemia or hyperlipidemia may have on ACR, all qualifying subjects will pass through a run-in phase of up to 3 months in duration, the aim of which is to improve glycemic and lipid control according to recommended guidelines. Similarly, hyperlipidemia has been implicated as contributing to renal dysfunction, as a consequence of an atherosclerotic and inflammatory process damaging the glomeruli and tubulo-interstitium.
- the run-in period will target: 1) Glucose control to at least ⁇ 8.0%, using dietary and lifestyle modifications plus oral agents and/or insulin; and 2) Control of LDL-cholesterol to ⁇ 100 mg/dL using dietary and lifestyle modifications plus HMG-CoA reductase inhibitor agents (statins) and/or ezetimibe.
- the run-in period will also be an opportunity to emphasize compliance with the subject's concurrent therapies, including their ACEI or ARB therapy. Up to 3 months will be permitted to achieve these goals, and the frequency of follow-up required to titrate therapy to meet these goals will be at the discretion of the investigator. Subjects who already meet these goals reliably may proceed to the baseline visit and randomization. Subjects who fail to meet both of these goals reliably after 3 months will be withdrawn, but may be re-screened at a later date if they can meet both goals at that time.
- Randomization Qualifying subjects who pass the run-in period will be randomized to receive either the indapamide and spironolactone combination or HCTZ, added to their previous therapy.
- Study Medications, Dose Titration, and Rescue Therapy Because all study medications in this open-label trial are FDA-approved for the management of hypertension, the subject will be given individual prescriptions (without refills). sufficient for 3 months at baseline and at 2-month intervals. All unused pills must be presented to the study coordinators and counted at each of the 2, 4, and 6-month visits to determine compliance, and an adequate supply for an additional 3-months will be provided at each of these visits to ensure the subject has an adequate supply. The subject's compliance with his/her pre-study ACEI or ARB agents and all other concurrent therapies will also be reviewed at these visits.
- Tier 1 will consist of indapamide 1.25 mg once daily together with spironolactone 25 mg once daily
- Tier 2 will consist of indapamide 2.5 mg once daily together with spironolactone 25 mg once daily.
- Tier 1 will consist of HCTZ 12.5 mg once daily, and Tier 2 will consist of HCTZ 25 mg once daily.
- BP remains ⁇ 130/80 mm Hg at the Month 2 visit after treatment with the Tier 2 dose
- subjects will be additionally prescribed clonidine, starting at 0.1 mg bid, titrating up to 0.3 mg bid, as tolerated; and/or guanfacine, starting at 1 mg qhs, titrating up to 3 mg qhs, as tolerated; until BP is controlled to ⁇ 130/80 mm Hg.
- Dose titrations of clonidine and/or guanfacine may occur more frequently than the scheduled visits, if necessary.
- dose reductions of anti-hypertensive medications will conform to the following sequence: 1) Taper the doses of any centrally-acting agent(s) (i.e., clonidine and/or guanfacine) or any concurrent calcium channel blocker agent, until symptoms of postural hypotension are eliminated; 2) If symptoms persist despite discontinuation of those agents, for subjects without a history of peripheral edema or CHF, lower the study medication dosage by one Tier at a time; or for subjects with a history of peripheral edema or CHF, lower the dose of the subject's ACEI or ARB agent by one half, until symptoms of postural hypotension are eliminated; 3) If symptoms persist despite complete discontinuation of the subject's study medications or ACEI/ARB agent, the subject should be withdrawn from any centrally-acting agent(s) (i.e., clonidine and/or guanfacine) or any concurrent calcium channel blocker agent, until symptoms of postural hypotension are eliminated; 2) If symptoms persist despite discontinuation of those
- ITT intent-to-treat
- PP per-protocol
- ITT analyses data from randomized subjects who fail to complete the study in its entirety will be imputed using a last-value-carried-forward (LVCF) approach based on their last known post-randomization values.
- LVCF last-value-carried-forward
- Non-normal variables will be transformed using an appropriate method or analyzed using equivalent non-parametric tests.
- Analyses of the study's key outcome parameters (ACR, systolic and diastolic BP, creatinine, eGFR using both methods, electrolytes, and clinical adverse events) will each be analyzed by repeated measures analysis of covariance (ANCOVA) to determine the between-group differences over time (group x time interaction, corrected for baseline), both as unadjusted analyses and after adjustment for the variables of age, gender, self-reported ethnicity (Hispanic vs. African-American vs. Other), changes in BMI, changes in HbA 1c , changes in LDL-cholesterol, and most importantly, the changes in systolic and diastolic BP.
- ACR systolic and diastolic BP
- creatinine eGFR using both methods, electrolytes, and clinical adverse events
- ANCOVA repeated measures analysis of covariance
- subjects will be stratified into subgroups based on: a) gender; b) ethnicity (African-Americans vs. Hispanics); c) microalbuminuria vs. macroalbuminuria (above vs. below 300 mg/gram creatinine); d) eGFR (above vs. below 60 mL/min); and e) baseline BP (above vs. below 130/80 mm Hg); and then analyzed separately to determine if any between-group differences in the study's key outcomes are more or less pronounced in these specific subgroups. All multivariate adjustments will be conducted using an appropriate linear regression model. Statistical significance will be p ⁇ 0.05.
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Claims (8)
- Verwendung von Indapamid für die Herstellung eines Medikaments zur gemeinsamen Verabreichung mit einem Anti-Aldosteron-Mittel zur Behandlung einer Erkrankung bei einer Zielperson, wobei das Anti-Aldosteron-Mittel Spironolacton oder Eplerenon ist, und wobei die Erkrankung Proteinurie, Albuminurie oder Hyperurikämie ist.
- Verwendung eines Anti-Aldosteron-Mittels für die Herstellung eines Medikaments zur gemeinsamen Verabreichung mit Indapamid zur Behandlung einer Erkrankung bei einer Zielperson, wobei das Anti-Aldosteron-Mittel Spironolacton oder Eplerenon ist, und wobei die Erkrankung Proteinurie, Albuminurie oder Hyperurikämie ist.
- Zusammensetzung, welche Indapamid und ein Anti-Aldosteron-Mittel umfasst, wobei das Anti-Aldosteron-Mittel Spironolacton oder Eplerenon ist.
- Verwendung nach einem der Ansprüche 1 und 2, wobei Indapamid und das Anti-Aldosteron-Mittel zur gleichzeitigen Verabreichung in einer einzigen Bereitstellungsträgersubstanz bereitgestellt werden.
- Verwendung nach Anspruch 4, wobei die einzige Bereitstellungsträgersubstanz so gestaltet ist, dass sie zur oralen Verabreichung dient.
- Verwendung nach einem der Ansprüche 1 oder 2, wobei Indapamid und das Anti-Aldosteron-Mittel durch mehr als eine Trägersubstanz bereitgestellt werden.
- Verwendung nach einem der Ansprüche 1, 2, 4 oder 6, wobei das Medikament außerdem einen Wirkstoff beinhaltet, welcher eine Funktion hat, die ausgewählt ist aus einer Gruppe, die das Verhindern oder Verringern von Proteinurie, die Förderung von Natriurese und das Verhindern oder Reduzieren von Hypertension umfasst.
- Verwendung nach Anspruch 7, wobei der Wirkstoff ausgewählt ist aus einer Gruppe, die Angiotensin-Konversions-Enzym-Hemmer, Anti-Renin-Mittel, Endothelin-Antagonisten, Calciumkanalblocker, Betablocker, Stickoxiddonoren, Ganglienblocker, Alpha-Methyl-Dopa, Alphablocker und entzündungshemmende Mittel umfasst.
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NZ606186A (en) * | 2010-06-24 | 2015-02-27 | Murray Goulburn Coop Co Ltd | Use of lactoferrin to treat proteinuria |
CN103120715B (zh) * | 2013-02-01 | 2015-02-04 | 广州中医药大学第二附属医院 | 一种用于制备防治局灶性肾小球硬化症药物的中药组合物 |
CN113082021A (zh) * | 2014-01-31 | 2021-07-09 | 詹森药业有限公司 | 用于治疗和预防肾病和脂肪肝病的方法 |
DK3358347T3 (da) * | 2015-09-30 | 2020-11-30 | Univ Tohoku | Markør til bestemmelse af diabetisk nefropati |
KR20180123021A (ko) * | 2016-03-24 | 2018-11-14 | 다이이찌 산쿄 가부시키가이샤 | 신질환의 치료를 위한 의약 |
GB201804515D0 (en) * | 2018-03-21 | 2018-05-02 | Takayuki Takakondo | Treatment of necroptosis |
US11202787B2 (en) | 2018-07-02 | 2021-12-21 | Corcept Therapeutics, Inc. | Use of ACTH in assessment and prophylactic treatment of hypokalemia associated with glucocorticoid receptor modulator treatment of Cushing's syndrome patients |
US10780097B2 (en) * | 2018-07-02 | 2020-09-22 | Corcept Therapeutics, Inc. | Use of cortisol in assessment and prophylactic treatment of hypokalemia associated with glucocorticoid receptor modulator treatment of Cushing's syndrome patients |
US10231983B1 (en) | 2018-08-22 | 2019-03-19 | Corcept Therapeutics, Inc. | Use of ACTH in assessment and prophylactic treatment of hypokalemia associated with glucocorticoid receptor modulator treatment of Cushing's syndrome patients |
WO2021058750A1 (en) * | 2019-09-27 | 2021-04-01 | Cardiorenal | Overall loop system |
CN112773871A (zh) * | 2021-01-29 | 2021-05-11 | 江阴市中医院 | 一种清化健脾方及用于制备预防结直肠腺瘤术后复发的药物的用途 |
CN112773877A (zh) * | 2021-01-29 | 2021-05-11 | 成都中医药大学附属医院 | 一种治疗糖尿病肾病蛋白尿的药物组合物及其制备方法和用途 |
CN113730520B (zh) * | 2021-09-30 | 2022-06-10 | 上海市第七人民医院(上海中医药大学附属第七人民医院) | 一种治疗糖尿病肾病蛋白尿的中药组合 |
CN115192563B (zh) * | 2022-05-09 | 2023-10-13 | 北京大学第一医院 | C3a/C3aR通路拮抗剂治疗原发性膜性肾病的用途 |
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Publication number | Priority date | Publication date | Assignee | Title |
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EP1136078A3 (de) * | 1995-02-10 | 2002-07-24 | G.D. Searle & Co. | Kombination von Angiotensin konvertierendem Enzym Hemmer und eine nebenwirkungsreduzierende Menge von Aldosteron Antagonist |
BR9915134A (pt) * | 1998-11-06 | 2001-08-07 | Searle & Co | Co-terapia e terapia combinada para o tratamento de distúrbio cardiovascular em um indivìduo, e, composição |
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JP2007230869A (ja) * | 2004-04-05 | 2007-09-13 | Takeda Chem Ind Ltd | アルドステロン受容体拮抗剤 |
US8173596B2 (en) * | 2004-05-14 | 2012-05-08 | The University Of North Carolina At Chapel Hill | Prouroguanylin, and synthetic analogs or proteolytic cleavage products derived from it, as therapeutic and diagnostic agents for diseases involving salt and/or fluid homeostasis |
WO2008124611A1 (en) * | 2007-04-05 | 2008-10-16 | Dr. Reddy's Laboratories Ltd. | Pharmaceutical compositions comprising ramipril and indapamide |
-
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Non-Patent Citations (3)
Title |
---|
BAKRIS G L ET AL: "Treatment of microalbuminuria in hypertensive subjects with elevated cardiovascular risk: results of the IMPROVE trial.", KIDNEY INTERNATIONAL OCT 2007, vol. 72, no. 7, October 2007 (2007-10-01), pages 879 - 885, ISSN: 0085-2538 * |
BOMBACK ANDREW S ET AL: "The incidence and implications of aldosterone breakthrough.", NATURE CLINICAL PRACTICE. NEPHROLOGY SEP 2007, vol. 3, no. 9, September 2007 (2007-09-01), pages 486 - 492, ISSN: 1745-8331 * |
MANN JOHANNES F E ET AL: "Renal outcomes with telmisartan, ramipril, or both, in people at high vascular risk (the ONTARGET study): a multicentre, randomised, double-blind, controlled trial.", LANCET 16 AUG 2008, vol. 372, no. 9638, 16 August 2008 (2008-08-16), pages 547 - 553, ISSN: 1474-547X * |
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CA2756779C (en) | 2019-10-29 |
CA2756779A1 (en) | 2010-09-30 |
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US20180243265A1 (en) | 2018-08-30 |
CN102421433B (zh) | 2015-09-23 |
US20100249081A1 (en) | 2010-09-30 |
WO2010111599A2 (en) | 2010-09-30 |
EP2411006A2 (de) | 2012-02-01 |
JP2012522006A (ja) | 2012-09-20 |
US20150258062A1 (en) | 2015-09-17 |
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AU2010229771A1 (en) | 2011-11-10 |
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